Department of Chemical & Biological Engineering, University of Wisconsin-Madison, 1415 Engineering Drive, Madison, Wisconsin 53706, United States.
Department of Chemistry, University of Wisconsin-Madison, 1101 University Avenue, Madison, Wisconsin 53706, United States.
ACS Infect Dis. 2023 Dec 8;9(12):2632-2651. doi: 10.1021/acsinfecdis.3c00468. Epub 2023 Nov 28.
Antimicrobial peptides (AMPs) are promising candidates to combat pathogens that are resistant to conventional antimicrobial drugs because they operate through mechanisms that involve membrane disruption. However, the use of AMPs in clinical settings has been limited, at least in part, by their susceptibility to proteolytic degradation and their lack of selectivity toward pathogenic microbes vs mammalian cells. We recently reported on the design of α- and β-peptide oligomers structurally templated upon the naturally occurring α-helical AMP aurein 1.2. These α/β-peptide oligomers are more proteolytically stable than aurein 1.2 and have several other attributes that render them attractive as alternatives to conventional AMPs. This study describes the influence of peptide physicochemical properties on the broad-spectrum activity of aurein 1.2-based α/β-peptide mimics against nine bacterial, fungal, and mammalian cell lines. We used a partial least-squares regression (PLSR)-supervised machine learning model to quantify and visualize relationships between experimentally determined physicochemical properties (e.g., hydrophobicity, charge, and helicity) and experimentally measured cell-type-specific activities of 21 peptides in a 149-member α/β-peptide library. Using this approach, we identified several peptides that were predicted to exhibit enhanced broad-spectrum selectivity, a measure that evaluates antimicrobial activity relative to mammalian cell toxicity compared to aurein 1.2. Experimental validation demonstrated high model predictive performance, and characterization of compounds with the highest broad-spectrum selectivity revealed peptide hydrophobicity, helicity, and helical rigidity to be strong predictors of broad-spectrum selectivity. The most selective peptide identified from the model prediction has more than a 13-fold improvement in broad-spectrum selectivity than that of aurein 1.2, demonstrating the ability of using PLSR models to identify quantitative structure-function relationships for nonstandard amino acid-containing peptides. Overall, this work establishes quantifiable guidelines for the rational design of helical antimicrobial α/β-peptides and identifies promising new α/β-peptides with significantly reduced mammalian toxicities and improved antifungal and antibacterial activities relative to aurein 1.2.
抗菌肽 (AMPs) 是对抗对抗生素药物具有耐药性的病原体的有前途的候选物,因为它们通过涉及破坏细胞膜的机制发挥作用。然而,由于 AMP 容易被蛋白水解降解,并且对致病微生物与哺乳动物细胞缺乏选择性,因此它们在临床环境中的应用受到限制。我们最近报道了基于天然存在的 α-螺旋 AMP aurein 1.2 设计的 α-和 β-肽寡聚物。与 aurein 1.2 相比,这些 α/β-肽寡聚物更具蛋白水解稳定性,并且具有其他一些特性,使其成为替代传统 AMP 的有吸引力的选择。本研究描述了肽理化性质对基于 aurein 1.2 的 α/β-肽模拟物广谱活性的影响,这些模拟物针对九种细菌、真菌和哺乳动物细胞系。我们使用偏最小二乘回归 (PLSR) 监督机器学习模型来量化和可视化实验确定的理化性质(例如疏水性、电荷和螺旋性)与 21 种肽在 149 种成员的 α/β-肽库中针对特定细胞类型的实验测定活性之间的关系。使用这种方法,我们确定了几种被预测具有增强的广谱选择性的肽,这种选择性衡量的是与 aurein 1.2 相比,抗微生物活性相对于哺乳动物细胞毒性的程度。实验验证证明了模型的高预测性能,并且对具有最高广谱选择性的化合物的表征表明,肽的疏水性、螺旋性和螺旋刚性是广谱选择性的强预测因子。从模型预测中鉴定出的最具选择性的肽与 aurein 1.2 的广谱选择性提高了 13 倍以上,证明了使用 PLSR 模型识别非标准氨基酸肽的定量结构-功能关系的能力。总体而言,这项工作为设计螺旋抗菌 α/β-肽建立了可量化的指南,并确定了具有显著降低哺乳动物毒性和提高抗真菌和抗菌活性的有前途的新型 α/β-肽,与 aurein 1.2 相比。
